We conducted a longitudinal cohort study to determine the association of Helicobacter pylori infection and the progression of chronic atrophic gastritis (CAG) with gastric cancer. A cohort of 4,655 healthy asymptomatic subjects was followed for a mean period of 7.7 years. H. pylori infection was established by serum specific antibodies and the presence of CAG was confirmed by serum pepsinogen. During the follow-up period, 45 gastric cancer cases were detected (incidence rate, 126/100,000 person-years). A univariate analysis after adjustment for age showed that both H. pylori and CAG were significantly associated with gastric cancer. Despite a worldwide decline in incidence, gastric cancer remains one of the leading causes of cancer-related death in Japan. [1][2][3][4] There is a marked geographic variability in the gastric cancer incidence rate; the cancer is most common in China and Japan, and one of the lowest rates is in the United States. [1][2][3][4] Many epidemiologic studies have shown that the risk of gastric cancer is strongly associated with environmental factors, such as salt, nitrates and low intake of fresh fruits and vegetables. 1,4 -8 Recent studies have indicated that Helicobacter pylori infection is also a major risk factor for the development of gastric cancer. 9 -18 The prevalence of H. pylori infection is markedly higher in Japan than in other industrialized countries, although the reasons are not fully understood. 19 -21 The observed geographic variability in gastric cancer appears to be explained by a synergistic interaction between H. pylori infection and other environmental factors.The H. pylori bacterium colonizes the stomach mucosa and triggers a series of inflammatory reactions. It is considered an important cause of chronic atrophic gastritis (CAG), 19 -23 as shown in rodent models. 24 -26 CAG is considered the first step of a sequence of mucosal changes in the stomach leading to cancer. The current model for stomach carcinogenesis begins with gastritis, proceeds to CAG, then to intestinal metaplasia, dysplasia and, finally, carcinoma. 1,27 This hypothesis is supported by a considerable number of clinicopathological and epidemiological studies in countries with a high incidence of gastric cancer. However, longitudinal cohort studies that report an association of CAG with gastric cancer and a relation between the progression of CAG and the development of gastric cancer are limited. 28 -30 In addition, the role of H. pylori infection in the above-mentioned process of stomach carcinogenesis remains unclear. To investigate these problems relating to gastric cancer development, we established a cohort of male factory workers that we followed prospectively for 8 years.CAG in a high-risk population, such as Japanese subjects, usually begins at the gastric antrum and extends proximally towards the cardia. [31][32][33] As a result, gastric secretory function diminishes as the area of functional fundic gland mucosa gets smaller. 34 CAG is a histopathological diagnosis. It is difficult, howe...
Our study investigated the relationship between gastric cancer development and activity of Helicobacter pylori-associated chronic gastritis or the resulting chronic atrophic gastritis (CAG). A cohort of 4,655 healthy asymptomatic subjects, in whom serum pepsinogen (PG) and H. pylori antibody titer had been measured to assess the activity and stage of H. pylori-associated chronic gastritis, was followed for up to 16 years, and cancer development was investigated. In subjects with a serologically diagnosed healthy stomach (H. pylori-negative/CAG-negative), cancer incidence rate was low, at 16/100,000 person-years. With the establishment of H. pylori infection and progression of chronic gastritis, significant stepwise cancer risk elevations were seen from CAG-free subjects (H. pylori-positive/CAG-negative) [hazard ratio (HR) 5 8.9, 95% confidence interval (CI) 5 2.7-54.7] to subjects with CAG (H. pylori-positive/CAG-positive) (HR 5 17.7, 95% CI 5 5.4-108.6) and finally to subjects with metaplastic gastritis (H. pylori-negative/CAG-positive) (HR 5 69.7, 95% CI 5 13.6-502.9). In H. pylori-infected CAG-free subjects, significantly elevated cancer risk was observed in the subgroup with active inflammation-based high PG II level or potent immune responsebased high H. pylori antibody titer; the former was associated with a particularly high risk of diffuse-type cancer, and both subgroups showed high cancer incidence rates of around 250/100,000 person-years, comparable to that in subjects with CAG. No such risk elevation was observed in H. pylori-infected subjects with CAG. These results clearly indicate that gastric cancer develops mainly from the gastritis-atrophy-metaplasia-cancer sequence and partly from active inflammation-based direct carcinogenesis, and that serum levels of PG and H. pylori antibody titer provide indices of cancer development in H. pylori-infected subjects.Despite worldwide declines in the incidence of gastric cancer and associated mortality over the past 50 years, this pathology remains one of the leading causes of cancer-related death in Eastern Asia, including Japan, South America and Eastern Europe.1-4 In Japan, more than 100,000 new cases of gastric cancer are diagnosed every year, and the Japanese Ministry of Health, Labor and Welfare reported that 50,136 deaths attributed to the cancer in 2010.5 Gastric cancer thus remains a major health problem in Japan. Development of gastric cancer represents a classical example of host-genetic and environmental interactions and is characterized by a multistep process of molecular and morphological events known as the gastritisatrophy-metaplasia-dysplasia-cancer sequence.6,7 Based on a large number of epidemiological and clinicopathological studies and also on animal experiments using Mongolian gerbils, this sequence, which predominantly leads to intestinal-type cancer, is considered to represent a major route of stomach carcinogenesis, particularly in areas of high cancer risk, such as Japan. Although other environmental and lifestyle factors together wi...
A longitudinal cohort study was conducted in Helicobactor pyloriinfected middle-aged Japanese males to evaluate the preventive effects of H. pylori eradication on the development of gastric cancer according to the extent of chronic atrophic gastritis (CAG). The extent of CAG was monitored by baseline serum pepsinogen (PG) levels. We followed 3,656 subjects with persistent H. pylori infection and 473 subjects with successful H. pylori eradication for cancer development for a mean (SD) of 9.3 (0.7) years. Groups with and without extensive CAG were categorized based on PG test-positive criteria to detect extensive CAG of PG I 70 ng/ml and PG I/II ratio 3.0. During the study period, 5 and 55 gastric cancers developed in H. pylori-eradicated and the noneradicated subjects, respectively, indicating no significant reduction in cancer incidence after H. pylori eradication. Among the noneradicated subjects, 1,329 were PG test-positive and 2,327 were PG test-negative. Gastric cancer was confirmed in 30 and 25 subjects, respectively. Among subjects whose infection was eradicated, 155 were PG test-positive and 318 were PG test-negative. Of these subjects, gastric cancer was confirmed in 3 and 2 subjects, respectively. Significant reduction in cancer incidence after eradication was observed only in PG test-negative subjects (p < 0.05; log-rank test). The results of this study strongly indicate that cancer development after eradication depends on the presence of extensive CAG before eradication and that H. pylori eradication is beneficial to most PG test-negative subjects with mild CAG as defined by the aforementioned criteria. ' 2009 UICC
Background: Gastric cancer screening using the pepsinogen filter test is receiving wide recognition in Japan owing to convenience, freedom from discomfort or risk, efficiency, and economy. Because the long-term outcomes of cancer development in extensive atrophic gastritis detected by pepsinogen test are unclear, testpositive and test-negative subjects were investigated in a longitudinal cohort study. Methods: Subjects comprised 5,209 middle-aged men with measured serum pepsinogen levels who were followed for 10 years. Cancer development based on ''atrophy-positive'' and ''atrophy-negative'' criteria used for cancer screening was investigated. Results: During the study, 63 cases of cancer developed in the cohort, representing an incidence rate of 125 per 100,000 person-years. Pepsinogen test screening using the most widely used atrophy-positive criterion (pepsinogen I, V70 ng/mL; pepsinogen I/II ratio, V3.0) displayed 58.7% sensitivity, 73.4% specificity, and 2.6% positive predictive value. Cancer inci-
BackgroundThrombocytopenia represents an obstacle for invasive procedures in chronic liver disease (CLD) patients. We aimed to estimate the appropriate dose and evaluate the efficacy and safety of lusutrombopag for the treatment of thrombocytopenia before percutaneous liver radiofrequency ablation (RFA) for primary hepatic cancer in patients with CLD.MethodsIn this multicenter, randomized, double-blind, placebo-controlled study conducted in Japan, 61 CLD patients with platelet count < 50 × 103/µL at screening were randomized to placebo or lusutrombopag 2, 3, or 4 mg once daily for 7 days, followed by a 28-day post-treatment assessment period. The primary efficacy endpoint was the proportion of patients who did not require platelet transfusion before RFA. The pre-specified key secondary efficacy endpoint was the proportion of responders. Adverse events (AEs) and thrombosis-related AEs were evaluated.ResultsThe proportion of patients who did not require platelet transfusion before RFA and that of responders were significantly higher (p < 0.01) in the 2-mg (80.0, 66.7%), 3-mg (81.3, 68.8%), and 4-mg groups (93.3, 80.0%) compared with the placebo group (20.0, 6.7%) and showed a dose-dependent effect. The incidence of AEs was 97.8 and 100% in the lusutrombopag (all groups) and placebo groups, respectively; no dose-related increase was observed. Four patients experienced thrombosis-related events (one each in the placebo and 2-mg groups, and two in the 4-mg group). A total of 16 (18%) adverse drug reactions occurred in the safety analysis set.ConclusionsLusutrombopag 3 mg once daily for 7 days was effective without raising concerns about excessive increases in platelet count.Clinical trial registrationThe study is registered at JapicCTI-121944.Electronic supplementary materialThe online version of this article (10.1007/s00535-018-1499-2) contains supplementary material, which is available to authorized users.
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